Author
Listed:
- Caeul Lim
(Harvard School of Public Health)
- Elsa Hansen
(Center for Communicable Disease Dynamics, Harvard School of Public Health)
- Tiffany M. DeSimone
(Harvard School of Public Health)
- Yovany Moreno
(Harvard School of Public Health)
- Klara Junker
(Harvard School of Public Health)
- Amy Bei
(Harvard School of Public Health)
- Carlo Brugnara
(Children’s Hospital Boston)
- Caroline O. Buckee
(Center for Communicable Disease Dynamics, Harvard School of Public Health
Harvard School of Public Health)
- Manoj T. Duraisingh
(Harvard School of Public Health)
Abstract
The macaque malaria parasite Plasmodium knowlesi has recently emerged as an important zoonosis in Southeast Asia. Infections are typically mild but can cause severe disease, achieving parasite densities similar to fatal Plasmodium falciparum infections. Here we show that a primate-adapted P. knowlesi parasite proliferates poorly in human blood due to a strong preference for young red blood cells (RBCs). We establish a continuous in vitro culture system by using human blood enriched for young cells. Mathematical modelling predicts that parasite adaptation for invasion of older RBCs is a likely mechanism leading to high parasite densities in clinical infections. Consistent with this model, we find that P. knowlesi can adapt to invade a wider age range of RBCs, resulting in proliferation in normal human blood. Such cellular niche expansion may increase pathogenesis in humans and will be a key feature to monitor as P. knowlesi emerges in human populations.
Suggested Citation
Caeul Lim & Elsa Hansen & Tiffany M. DeSimone & Yovany Moreno & Klara Junker & Amy Bei & Carlo Brugnara & Caroline O. Buckee & Manoj T. Duraisingh, 2013.
"Expansion of host cellular niche can drive adaptation of a zoonotic malaria parasite to humans,"
Nature Communications, Nature, vol. 4(1), pages 1-9, June.
Handle:
RePEc:nat:natcom:v:4:y:2013:i:1:d:10.1038_ncomms2612
DOI: 10.1038/ncomms2612
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